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新生儿及婴儿期发病糖尿病的诊断

Diagnosis of neonatal and infancy-onset diabetes.

作者信息

Barbetti Fabrizio

机构信息

San Raffaele Biomedical Park Foundation and Bambino Gesù Pediatric Hospital and Department of Internal Medicine, University of Tor Vergata, Rome, Italy.

出版信息

Endocr Dev. 2007;11:83-93. doi: 10.1159/000111060.

Abstract

Until 1995, the etiology of 'neonatal' diabetes was totally unknown. In about a decade, mutations in 8 different genes (IPF1, EIF2AK3, GK, FOXP3, KCNJ11, ABCC8, PTF1A and GLIS3) have been discovered in patients with the permanent form of the disease, and 3 genetic abnormalities (defects in the paternally imprinted chromosomal region 6q24 and 'mild' activating mutations in KCNJ11 or ABCC8) have been detected in subjects with transient neonatal diabetes. Together with the advances in the understanding of the pathophysiology of this condition, clearly different from type 1 diabetes, also the temporal criterion by which one clinically defines a patient as being affected by neonatal diabetes has changed. In 1995, neonatal diabetes was defined as hyperglycemia that requires insulin treatment and occurs during the first month of life. In some patients with defects of KCNJ11, ABCC8 or EIF2AK3 genes however, diabetes can present at 6 months of age and beyond. It is now time to adopt a new definition in order to avoid the confusion originating by the misuse of the term 'neonatal'. I would suggest monogenic diabetes of infancy, which includes both the permanent and the transient types, irrespectively of the mechanism of disease.

摘要

直到1995年,“新生儿”糖尿病的病因完全不明。在大约十年时间里,已在永久性形式疾病患者中发现8种不同基因(IPF1、EIF2AK3、GK、FOXP3、KCNJ11、ABCC8、PTF1A和GLIS3)发生突变,并且在短暂性新生儿糖尿病患者中检测到3种基因异常(父系印记染色体区域6q24缺陷以及KCNJ11或ABCC8中的“轻度”激活突变)。随着对这种明显不同于1型糖尿病的病症病理生理学认识的进展,临床上将患者定义为患有新生儿糖尿病的时间标准也发生了变化。1995年,新生儿糖尿病被定义为需要胰岛素治疗且在出生后第一个月内发生的高血糖症。然而,在一些KCNJ11、ABCC8或EIF2AK3基因缺陷患者中,糖尿病可在6个月及以后出现。现在是时候采用新定义以避免因滥用“新生儿”一词而产生的混淆了。我建议采用婴儿单基因糖尿病这一术语,它包括永久性和短暂性两种类型,而不考虑疾病机制。

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